Innate αβ T cells mediate antitumor immunity by orchestrating immunogenic macrophage programming

Mautin Hundeyin; Emma Kurz; Ankita Mishra; Juan Andres Kochen Rossi; Shannon M. Liudahl; Kenna R. Leis; Harshita Mehrotra; Mirhee Kim; Luisana E. Torres; Adesola Ogunsakin; Jason Link; Rosalie C. Sears; Shamilene Sivagnanam; Jeremy Goecks; K. M.Sadeq Islam; Igor Dolgalev; Shivraj Savadkar; Wei Wang; Berk Aykut; Joshua Leinwand; Brian Diskin; Salma Adam; Muhammad Israr; Maeliss Gelas; Justin Lish; Kathryn Chin; Mohammad Saad Farooq; Benjamin Wadowski; Jingjing Wu; Suhagi Shah; Dennis O. Adeegbe; Smruti Pushalkar; Varshini Vasudevaraja; Deepak Saxena; Kwok Kin Wong; Lisa M. Coussens; George Miller

doi:10.1158/2159-8290.CD-19-0161

Innate αβ T cells mediate antitumor immunity by orchestrating immunogenic macrophage programming

Mautin Hundeyin, Emma Kurz, Ankita Mishra, Juan Andres Kochen Rossi, Shannon M. Liudahl, Kenna R. Leis, Harshita Mehrotra, Mirhee Kim, Luisana E. Torres, Adesola Ogunsakin, Jason Link, Rosalie C. Sears, Shamilene Sivagnanam, Jeremy Goecks, K. M.Sadeq Islam, Igor Dolgalev, Shivraj Savadkar, Wei Wang, Berk Aykut, Joshua LeinwandBrian Diskin, Salma Adam, Muhammad Israr, Maeliss Gelas, Justin Lish, Kathryn Chin, Mohammad Saad Farooq, Benjamin Wadowski, Jingjing Wu, Suhagi Shah, Dennis O. Adeegbe, Smruti Pushalkar, Varshini Vasudevaraja, Deepak Saxena, Kwok Kin Wong, Lisa M. Coussens, George Miller

Research output: Contribution to journal › Article › peer-review

16 Scopus citations

Abstract

Unconventional T-lymphocyte populations are emerging as important regulators of tumor immunity. Despite this, the role of TCRαβ⁺CD4^-CD8^-NK1.1^- innate αβ T cells (iαβT) in pancreatic ductal adenocarcinoma (PDA) has not been explored. We found that iαβTs represent ∼10% of T lymphocytes infiltrating PDA in mice and humans. Intratumoral iαβTs express a distinct T-cell receptor repertoire and profoundly immunogenic phenotype compared with their peripheral counterparts and conventional lymphocytes. iαβTs comprised ∼75% of the total intratumoral IL17⁺ cells. Moreover, iαβT-cell adoptive transfer is protective in both murine models of PDA and human organotypic systems. We show that iαβT cells induce a CCR5-dependent immunogenic macrophage reprogramming, thereby enabling marked CD4⁺ and CD8⁺ T-cell expansion/activation and tumor protection. Collectively, iαβTs govern fundamental intratumoral cross-talk between innate and adaptive immune populations and are attractive therapeutic targets. SIGNIFICANCE: We found that iαβTs are a profoundly activated T-cell subset in PDA that slow tumor growth in murine and human models of disease. iαβTs induce a CCR5-dependent immunogenic tumor-associated macrophage program, T-cell activation and expansion, and should be considered as novel targets for immunotherapy.

Original language	English (US)
Pages (from-to)	1288-1305
Number of pages	18
Journal	Cancer discovery
Volume	9
Issue number	9
DOIs	https://doi.org/10.1158/2159-8290.CD-19-0161
State	Published - 2019

ASJC Scopus subject areas

Oncology

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10.1158/2159-8290.CD-19-0161

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Hundeyin, M., Kurz, E., Mishra, A., Rossi, J. A. K., Liudahl, S. M., Leis, K. R., Mehrotra, H., Kim, M., Torres, L. E., Ogunsakin, A., Link, J., Sears, R. C., Sivagnanam, S., Goecks, J., Islam, K. M. S., Dolgalev, I., Savadkar, S., Wang, W., Aykut, B., ... Miller, G. (2019). Innate αβ T cells mediate antitumor immunity by orchestrating immunogenic macrophage programming. Cancer discovery, 9(9), 1288-1305. https://doi.org/10.1158/2159-8290.CD-19-0161

Hundeyin, M, Kurz, E, Mishra, A, Rossi, JAK, Liudahl, SM, Leis, KR, Mehrotra, H, Kim, M, Torres, LE, Ogunsakin, A, Link, J, Sears, RC, Sivagnanam, S, Goecks, J, Islam, KMS, Dolgalev, I, Savadkar, S, Wang, W, Aykut, B, Leinwand, J, Diskin, B, Adam, S, Israr, M, Gelas, M, Lish, J, Chin, K, Farooq, MS, Wadowski, B, Wu, J, Shah, S, Adeegbe, DO, Pushalkar, S, Vasudevaraja, V, Saxena, D, Wong, KK, Coussens, LM & Miller, G 2019, 'Innate αβ T cells mediate antitumor immunity by orchestrating immunogenic macrophage programming', Cancer discovery, vol. 9, no. 9, pp. 1288-1305. https://doi.org/10.1158/2159-8290.CD-19-0161

@article{bafce6656132431b80767b346f3de45d,

title = "Innate αβ T cells mediate antitumor immunity by orchestrating immunogenic macrophage programming",

abstract = "Unconventional T-lymphocyte populations are emerging as important regulators of tumor immunity. Despite this, the role of TCRαβ+CD4-CD8-NK1.1- innate αβ T cells (iαβT) in pancreatic ductal adenocarcinoma (PDA) has not been explored. We found that iαβTs represent ∼10% of T lymphocytes infiltrating PDA in mice and humans. Intratumoral iαβTs express a distinct T-cell receptor repertoire and profoundly immunogenic phenotype compared with their peripheral counterparts and conventional lymphocytes. iαβTs comprised ∼75% of the total intratumoral IL17+ cells. Moreover, iαβT-cell adoptive transfer is protective in both murine models of PDA and human organotypic systems. We show that iαβT cells induce a CCR5-dependent immunogenic macrophage reprogramming, thereby enabling marked CD4+ and CD8+ T-cell expansion/activation and tumor protection. Collectively, iαβTs govern fundamental intratumoral cross-talk between innate and adaptive immune populations and are attractive therapeutic targets. SIGNIFICANCE: We found that iαβTs are a profoundly activated T-cell subset in PDA that slow tumor growth in murine and human models of disease. iαβTs induce a CCR5-dependent immunogenic tumor-associated macrophage program, T-cell activation and expansion, and should be considered as novel targets for immunotherapy.",

author = "Mautin Hundeyin and Emma Kurz and Ankita Mishra and Rossi, {Juan Andres Kochen} and Liudahl, {Shannon M.} and Leis, {Kenna R.} and Harshita Mehrotra and Mirhee Kim and Torres, {Luisana E.} and Adesola Ogunsakin and Jason Link and Sears, {Rosalie C.} and Shamilene Sivagnanam and Jeremy Goecks and Islam, {K. M.Sadeq} and Igor Dolgalev and Shivraj Savadkar and Wei Wang and Berk Aykut and Joshua Leinwand and Brian Diskin and Salma Adam and Muhammad Israr and Maeliss Gelas and Justin Lish and Kathryn Chin and Farooq, {Mohammad Saad} and Benjamin Wadowski and Jingjing Wu and Suhagi Shah and Adeegbe, {Dennis O.} and Smruti Pushalkar and Varshini Vasudevaraja and Deepak Saxena and Wong, {Kwok Kin} and Coussens, {Lisa M.} and George Miller",

note = "Funding Information: This work was supported by NIH grants CA168611 (G. Miller), CA203105 (G. Miller), CA215471 (G. Miller), CA19311 (G. Miller), and DK106025 (G. Miller), the Knight Cancer Institute NCI P30 CA069533 (L.M. Coussens and R.C. Sears), the Brenden-Colson Center for Pancreatic Care (L.M. Coussens, S.M. Liudahl, K.R. Leis, J. Link, R.C. Sears, S. Sivagnanam, J. Goecks), Stand Up To Cancer– Lustgarten Foundation, Pancreatic Cancer Convergence Dream Team Translational Research Grant (SU2-AACR-DT14-14; L.M. Coussens and S.M. Liudahl), Stand Up To Cancer (SU2C) is a Division of the Entertainment Industry Foundation administered by the American Association for Cancer Research, the Scientific Partner of SU2C; and a resident research fellowship from the American Society for Colorectal Surgery (M. Hundeyin). Funding Information: D. Saxena has ownership interest (including stock, patents, etc.) in Periomicscare LLC. L.M. Coussens reports receiving commercial research grants from Acerta Pharma, LLC, Deciphera Pharmaceuticals, Roche Glycart AG, and Syndax Pharmaceuticals, Inc.; reports receiving other commercial research support from Plexxikon Inc, Pharmacyclics, Inc., Acerta Pharma, LLC, Deciphera Pharmaceuticals, Genentech, Inc., Roche Glycart AG, Cell Signaling Technologies, and NanoString Technologies, Inc.; is a member of the Pharmacy-clics, Inc. steering committee for PCYC-1137-CA (NCT02436668); and is a consultant/advisory board member for Syndax Pharmaceuticals, Inc., Cancer Research Institute (CRI), The V Foundation for Cancer Research, Cancer Research United Kingdom (CRUK) Early Detection (EDx) Research Committee, Starr Cancer Consortium, NIH/NCI-Frederick National Laboratory Advisory Committee (FNLAC), Cell Signaling Technologies, Carisma Therapeutics Inc., Verseau Therapeutics, Inc., Zymeworks, Inc., (P30) Melvin and Bren Simon Cancer Center, Indiana University, (P30) Koch Institute for Integrated Cancer Research, Massachusetts Institute of Technology, (P30) Salk Institute Cancer Center, Bloomberg-Kimmel Institute for Cancer Immunotherapy, Sidney Kimmel Comprehensive Cancer Center at Johns Hopkins, and Dana-Farber Cancer Center Breast SPORE. No potential conflicts of interest were disclosed by the other authors. Publisher Copyright: {\textcopyright} 2019 American Association for Cancer Research.",

year = "2019",

doi = "10.1158/2159-8290.CD-19-0161",

language = "English (US)",

volume = "9",

pages = "1288--1305",

journal = "Cancer discovery",

issn = "2159-8274",

publisher = "American Association for Cancer Research Inc.",

number = "9",

}

TY - JOUR

T1 - Innate αβ T cells mediate antitumor immunity by orchestrating immunogenic macrophage programming

AU - Hundeyin, Mautin

AU - Kurz, Emma

AU - Mishra, Ankita

AU - Rossi, Juan Andres Kochen

AU - Liudahl, Shannon M.

AU - Leis, Kenna R.

AU - Mehrotra, Harshita

AU - Kim, Mirhee

AU - Torres, Luisana E.

AU - Ogunsakin, Adesola

AU - Link, Jason

AU - Sears, Rosalie C.

AU - Sivagnanam, Shamilene

AU - Goecks, Jeremy

AU - Islam, K. M.Sadeq

AU - Dolgalev, Igor

AU - Savadkar, Shivraj

AU - Wang, Wei

AU - Aykut, Berk

AU - Leinwand, Joshua

AU - Diskin, Brian

AU - Adam, Salma

AU - Israr, Muhammad

AU - Gelas, Maeliss

AU - Lish, Justin

AU - Chin, Kathryn

AU - Farooq, Mohammad Saad

AU - Wadowski, Benjamin

AU - Wu, Jingjing

AU - Shah, Suhagi

AU - Adeegbe, Dennis O.

AU - Pushalkar, Smruti

AU - Vasudevaraja, Varshini

AU - Saxena, Deepak

AU - Wong, Kwok Kin

AU - Coussens, Lisa M.

AU - Miller, George

N1 - Funding Information: This work was supported by NIH grants CA168611 (G. Miller), CA203105 (G. Miller), CA215471 (G. Miller), CA19311 (G. Miller), and DK106025 (G. Miller), the Knight Cancer Institute NCI P30 CA069533 (L.M. Coussens and R.C. Sears), the Brenden-Colson Center for Pancreatic Care (L.M. Coussens, S.M. Liudahl, K.R. Leis, J. Link, R.C. Sears, S. Sivagnanam, J. Goecks), Stand Up To Cancer– Lustgarten Foundation, Pancreatic Cancer Convergence Dream Team Translational Research Grant (SU2-AACR-DT14-14; L.M. Coussens and S.M. Liudahl), Stand Up To Cancer (SU2C) is a Division of the Entertainment Industry Foundation administered by the American Association for Cancer Research, the Scientific Partner of SU2C; and a resident research fellowship from the American Society for Colorectal Surgery (M. Hundeyin). Funding Information: D. Saxena has ownership interest (including stock, patents, etc.) in Periomicscare LLC. L.M. Coussens reports receiving commercial research grants from Acerta Pharma, LLC, Deciphera Pharmaceuticals, Roche Glycart AG, and Syndax Pharmaceuticals, Inc.; reports receiving other commercial research support from Plexxikon Inc, Pharmacyclics, Inc., Acerta Pharma, LLC, Deciphera Pharmaceuticals, Genentech, Inc., Roche Glycart AG, Cell Signaling Technologies, and NanoString Technologies, Inc.; is a member of the Pharmacy-clics, Inc. steering committee for PCYC-1137-CA (NCT02436668); and is a consultant/advisory board member for Syndax Pharmaceuticals, Inc., Cancer Research Institute (CRI), The V Foundation for Cancer Research, Cancer Research United Kingdom (CRUK) Early Detection (EDx) Research Committee, Starr Cancer Consortium, NIH/NCI-Frederick National Laboratory Advisory Committee (FNLAC), Cell Signaling Technologies, Carisma Therapeutics Inc., Verseau Therapeutics, Inc., Zymeworks, Inc., (P30) Melvin and Bren Simon Cancer Center, Indiana University, (P30) Koch Institute for Integrated Cancer Research, Massachusetts Institute of Technology, (P30) Salk Institute Cancer Center, Bloomberg-Kimmel Institute for Cancer Immunotherapy, Sidney Kimmel Comprehensive Cancer Center at Johns Hopkins, and Dana-Farber Cancer Center Breast SPORE. No potential conflicts of interest were disclosed by the other authors. Publisher Copyright: © 2019 American Association for Cancer Research.

PY - 2019

Y1 - 2019

N2 - Unconventional T-lymphocyte populations are emerging as important regulators of tumor immunity. Despite this, the role of TCRαβ+CD4-CD8-NK1.1- innate αβ T cells (iαβT) in pancreatic ductal adenocarcinoma (PDA) has not been explored. We found that iαβTs represent ∼10% of T lymphocytes infiltrating PDA in mice and humans. Intratumoral iαβTs express a distinct T-cell receptor repertoire and profoundly immunogenic phenotype compared with their peripheral counterparts and conventional lymphocytes. iαβTs comprised ∼75% of the total intratumoral IL17+ cells. Moreover, iαβT-cell adoptive transfer is protective in both murine models of PDA and human organotypic systems. We show that iαβT cells induce a CCR5-dependent immunogenic macrophage reprogramming, thereby enabling marked CD4+ and CD8+ T-cell expansion/activation and tumor protection. Collectively, iαβTs govern fundamental intratumoral cross-talk between innate and adaptive immune populations and are attractive therapeutic targets. SIGNIFICANCE: We found that iαβTs are a profoundly activated T-cell subset in PDA that slow tumor growth in murine and human models of disease. iαβTs induce a CCR5-dependent immunogenic tumor-associated macrophage program, T-cell activation and expansion, and should be considered as novel targets for immunotherapy.

AB - Unconventional T-lymphocyte populations are emerging as important regulators of tumor immunity. Despite this, the role of TCRαβ+CD4-CD8-NK1.1- innate αβ T cells (iαβT) in pancreatic ductal adenocarcinoma (PDA) has not been explored. We found that iαβTs represent ∼10% of T lymphocytes infiltrating PDA in mice and humans. Intratumoral iαβTs express a distinct T-cell receptor repertoire and profoundly immunogenic phenotype compared with their peripheral counterparts and conventional lymphocytes. iαβTs comprised ∼75% of the total intratumoral IL17+ cells. Moreover, iαβT-cell adoptive transfer is protective in both murine models of PDA and human organotypic systems. We show that iαβT cells induce a CCR5-dependent immunogenic macrophage reprogramming, thereby enabling marked CD4+ and CD8+ T-cell expansion/activation and tumor protection. Collectively, iαβTs govern fundamental intratumoral cross-talk between innate and adaptive immune populations and are attractive therapeutic targets. SIGNIFICANCE: We found that iαβTs are a profoundly activated T-cell subset in PDA that slow tumor growth in murine and human models of disease. iαβTs induce a CCR5-dependent immunogenic tumor-associated macrophage program, T-cell activation and expansion, and should be considered as novel targets for immunotherapy.

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U2 - 10.1158/2159-8290.CD-19-0161

DO - 10.1158/2159-8290.CD-19-0161

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AN - SCOPUS:85071783213

SN - 2159-8274

VL - 9

SP - 1288

EP - 1305

JO - Cancer discovery

JF - Cancer discovery

IS - 9

ER -

Innate αβ T cells mediate antitumor immunity by orchestrating immunogenic macrophage programming

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